Tanji Nozomu, Markowitz Glen S, Fu Caifeng, Kislinger Thomas, Taguchi Akihiko, Pischetsrieder Monika, Stern David, Schmidt Ann Marie, D'Agati Vivette D
Department of Pathology, Columbia University College of Physicians and Surgeons, New York, New York.
Department of Physiology, Columbia University College of Physicians and Surgeons, New York, New York.
J Am Soc Nephrol. 2000 Sep;11(9):1656-1666. doi: 10.1681/ASN.V1191656.
Advanced glycation end products (AGE) contribute to diabetic tissue injury by two major mechanisms, i.e., the alteration of extracellular matrix architecture through nonenzymatic glycation, with formation of protein crosslinks, and the modulation of cellular functions through interactions with specific cell surface receptors, the best characterized of which is the receptor for AGE (RAGE). Recent evidence suggests that the AGE-RAGE interaction may also be promoted by inflammatory processes and oxidative cellular injury. To characterize the distributions of AGE and RAGE in diabetic kidneys and to determine their specificity for diabetic nephropathy, an immunohistochemical analysis of renal biopsies from patients with diabetic nephropathy (n = 26), hypertensive nephrosclerosis (n = 7), idiopathic focal segmental glomerulosclerosis (n = 11), focal sclerosis secondary to obesity (n = 7), and lupus nephritis (n = 11) and from normal control subjects (n = 2) was performed, using affinity-purified antibodies raised to RAGE and two subclasses of AGE, i.e., N(epsilon)-(carboxymethyl)-lysine (CML) and pentosidine (PENT). AGE were detected equally in diffuse and nodular diabetic nephropathy. CML was the major AGE detected in diabetic mesangium (96%), glomerular basement membranes (GBM) (42%), tubular basement membranes (85%), and vessel walls (96%). In diabetic nephropathy, PENT was preferentially located in interstitial collagen (90%) and was less consistently observed in vessel walls (54%), mesangium (77%), GBM (4%), and tubular basement membranes (31%). RAGE was expressed on normal podocytes and was upregulated in diabetic nephropathy. The restriction of RAGE mRNA expression to glomeruli was confirmed by reverse transcription-PCR analysis of microdissected renal tissue compartments. The extent of mesangial and GBM immunoreactivity for CML, but not PENT, was correlated with the severity of diabetic glomerulosclerosis, as assessed pathologically. CML and PENT were also identified in areas of glomerulosclerosis and arteriosclerosis in idiopathic and secondary focal segmental glomerulosclerosis, hypertensive nephrosclerosis, and lupus nephritis. In active lupus nephritis, CML and PENT were detected in the proliferative glomerular tufts and crescents. In conclusion, CML is a major AGE in renal basement membranes in diabetic nephropathy, and its accumulation involves upregulation of RAGE on podocytes. AGE are also accumulated in acute inflammatory glomerulonephritis secondary to systemic lupus erythematosus, possibly via enzymatic oxidation of glomerular matrix proteins.
晚期糖基化终末产物(AGE)通过两种主要机制导致糖尿病组织损伤,即通过非酶糖基化改变细胞外基质结构,形成蛋白质交联,以及通过与特定细胞表面受体相互作用调节细胞功能,其中最具特征的是AGE受体(RAGE)。最近的证据表明,炎症过程和细胞氧化损伤也可能促进AGE-RAGE相互作用。为了表征AGE和RAGE在糖尿病肾脏中的分布,并确定它们对糖尿病肾病的特异性,我们使用针对RAGE和两种AGE亚类(即N(ε)-(羧甲基)-赖氨酸(CML)和戊糖苷(PENT))制备的亲和纯化抗体,对糖尿病肾病患者(n = 26)、高血压性肾硬化患者(n = 7)、特发性局灶节段性肾小球硬化患者(n = 11)、肥胖继发的局灶性硬化患者(n = 7)、狼疮性肾炎患者(n = 11)以及正常对照受试者(n = 2)的肾活检组织进行了免疫组织化学分析。在弥漫性和结节性糖尿病肾病中均检测到AGE。CML是在糖尿病系膜(96%)、肾小球基底膜(GBM)(42%)、肾小管基底膜(85%)和血管壁(96%)中检测到的主要AGE。在糖尿病肾病中,PENT优先位于间质胶原中(90%),在血管壁(54%)、系膜(77%)、GBM(4%)和肾小管基底膜(31%)中观察到的一致性较低。RAGE在正常足细胞上表达,在糖尿病肾病中上调。通过对显微切割的肾组织区室进行逆转录 - PCR分析,证实了RAGE mRNA表达仅限于肾小球。病理评估显示,CML而非PENT的系膜和GBM免疫反应程度与糖尿病肾小球硬化的严重程度相关。在特发性和继发性局灶节段性肾小球硬化、高血压性肾硬化和狼疮性肾炎的肾小球硬化和动脉硬化区域也鉴定出了CML和PENT。在活动性狼疮性肾炎中,在增殖性肾小球小叶和新月体中检测到CML和PENT。总之,CML是糖尿病肾病肾基底膜中的主要AGE,其积累涉及足细胞上RAGE的上调。AGE也可能通过肾小球基质蛋白的酶促氧化作用,在系统性红斑狼疮继发的急性炎症性肾小球肾炎中积累。
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